PRED-TMBB: a web server for predicting the topology of  -barrel outer membrane proteins

Bagos, Pantelis G.; Liakopoulos, Theodore D.; Spyropoulos, Ioannis C.; Hamodrakas, Stavros J.

doi:10.1093/nar/gkh417

Cited by 341 publications

(267 citation statements)

References 21 publications

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“…The PRED-TMBB program (40,41) predicts that these proteins form ␤-barrels with large periplasmic plugs of 152 residues and 201 residues for FslE and FupA, respectively. Our studies with 55 Fe transport in conjunction with the predicted structure of the proteins have confirmed the role of FslE as the siderophore receptor and identified FupA as a high affinity ferrous iron transporter in Schu S4.…”

Section: Discussionmentioning

confidence: 99%

Paralogous Outer Membrane Proteins Mediate Uptake of Different Forms of Iron and Synergistically Govern Virulence in Francisella tularensis tularensis

Ramakrishnan

Sen

Johnson

2012

Journal of Biological Chemistry

122

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Background: FslE and FupA are Francisella-specific paralogous proteins involved in iron acquisition. Results: fslE mutation disrupts siderophore-mediated ferric iron uptake, fupA mutation impairs high affinity ferrous iron uptake, and both mutations impact virulence. Conclusion: Optimal iron acquisition and virulence require both paralogs. Significance: Iron acquisition mechanisms are potential targets for preventive or therapeutic intervention in F. tularensis infections.

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Section: Discussionmentioning

confidence: 99%

Paralogous Outer Membrane Proteins Mediate Uptake of Different Forms of Iron and Synergistically Govern Virulence in Francisella tularensis tularensis

Ramakrishnan

Sen

Johnson

2012

Journal of Biological Chemistry

122

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“…HmsH is predicted to form a b-barrel protein with a large Nterminal periplasmic domain (Bagos et al, 2004;Kirillina et al, 2004). Our mutagenesis study concentrated on this periplasmic domain to avoid a loss of phenotype due to disruption of the b-barrel structure.…”

Section: Discussionmentioning

confidence: 99%

Identification of critical amino acid residues in the plague biofilm Hms proteins

et al. 2006

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Yersinia pestis biofilm formation causes massive adsorption of haemin or Congo red in vitro as well as colonization and eventual blockage of the flea proventriculus in vivo. This blockage allows effective transmission of plague from some fleas, like the oriental rat flea, to mammals. Four Hms proteins, HmsH, HmsF, HmsR and HmsS, are essential for biofilm formation, with HmsT and HmsP acting as positive and negative regulators, respectively. HmsH has a β-barrel structure with a large periplasmic domain while HmsF possesses polysaccharide deacetylase and COG1649 domains. HmsR is a putative glycosyltransferase while HmsS has no recognized domains. In this study, specific amino acids within conserved domains or within regions of high similarity in HmsH, HmsF, HmsR and HmsS proteins were selected for site-directed mutagenesis. Some but not all of the substitutions in HmsS and within the periplasmic domain of HmsH were critical for protein function. Substitutions within the glycosyltransferase domain of HmsR and the deacetylase domain of HmsF abolished biofilm formation in Y. pestis. Surprisingly, substitution of highly conserved residues within COG1649 did not affect HmsF function.

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“…Bagos et al assessed the ability of the methods to predict the location of the TM regions of beta-strands, as determined by PDB_TM (94). With the above factors as caveats, the study made one major conclusion: the top three methods namely, HMM-B2TMR (95), ProfTMB (93) and PRED-TMBB (91), are HMM-based and far outperform NN-and SVM-based methods in predicting topology and number of strands correctly.…”

Section: Prediction Of Tm Segmentsmentioning

confidence: 99%

“…http://www.bioinfo.no/tools/bomp WP PRED-TMBB (91) http://bioinformatics2.biol.uoa.gr/PRED-TMBB PR3 PROFtmb (93) http://rostlab.org/services/proftmb PR3, WP TMB-HUNT (156,157) http://www.bioinformatics.leeds.ac.uk/ WP * The methods in this Table are recommended either because they stood out in independent assessments or because otherwise interesting. See Table 3 for legend.…”

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confidence: 99%

Membrane protein prediction methods

Punta

Forrest

Bigelow

et al. 2007

Methods

109

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We survey computational approaches that tackle membrane protein structure and function prediction. While describing the main ideas that have led to the development of the most relevant and novel methods, we also discuss pitfalls, provide practical hints and highlight the challenges that remain. The methods covered include: sequence alignment, motif search, functional residue identification, transmembrane segment and protein topology predictions, homology and ab initio modeling. Overall, predictions of functional and structural features of membrane proteins are improving, although progress is hampered by the limited amount of high-resolution experimental information available. While predictions of transmembrane segments and protein topology rank among the most accurate methods in computational biology, more attention and effort will be required in the future to ameliorate database search, homology and ab initio modeling.

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PRED-TMBB: a web server for predicting the topology of -barrel outer membrane proteins

Cited by 341 publications

References 21 publications

Paralogous Outer Membrane Proteins Mediate Uptake of Different Forms of Iron and Synergistically Govern Virulence in Francisella tularensis tularensis

Paralogous Outer Membrane Proteins Mediate Uptake of Different Forms of Iron and Synergistically Govern Virulence in Francisella tularensis tularensis

Identification of critical amino acid residues in the plague biofilm Hms proteins

Membrane protein prediction methods

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